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通过易于聚集的结构域调节突触 pumilio 的功能。

Regulation of synaptic Pumilio function by an aggregation-prone domain.

机构信息

Division of Biology, California Institute of Technology, Pasadena, California 91125, USA.

出版信息

J Neurosci. 2010 Jan 13;30(2):515-22. doi: 10.1523/JNEUROSCI.2523-09.2010.

DOI:10.1523/JNEUROSCI.2523-09.2010
PMID:20071514
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2847508/
Abstract

We identified Pumilio (Pum), a Drosophila translational repressor, in a computational search for metazoan proteins whose activities might be regulated by assembly into ordered aggregates. The search algorithm was based on evolutionary sequence conservation patterns observed for yeast prion proteins, which contain aggregation-prone glutamine/asparagine (Q/N)-rich domains attached to functional domains of normal amino acid composition. We examined aggregation of Pum and its nematode ortholog PUF-9 by expression in yeast. A domain of Pum containing the Q/N-rich sequence, denoted as NQ1, the entire Pum N terminus, and the complete PUF-9 protein localize to macroscopic aggregates (foci) in yeast. NQ1 and PUF-9 can generate the yeast Pin+ trait, which is transmitted by a heritable aggregate. NQ1 also assembles into amyloid fibrils in vitro. In Drosophila, Pum regulates postsynaptic translation at neuromuscular junctions (NMJs). To assess whether NQ1 affects synaptic Pum activity in vivo, we expressed it in muscles. We found that it negatively regulates endogenous Pum, producing gene dosage-dependent pum loss-of-function NMJ phenotypes. NQ1 coexpression also suppresses lethality and NMJ phenotypes caused by overexpression of Pum in muscles. The Q/N block of NQ1 is required for these phenotypic effects. Negative regulation of Pum by NQ1 might be explained by formation of inactive aggregates, but we have been unable to demonstrate that NQ1 aggregates in Drosophila. NQ1 could also regulate Pum by a "dominant-negative" effect, in which it would block Q/N-mediated interactions of Pum with itself or with cofactors required for translational repression.

摘要

我们通过计算搜索,鉴定了一种果蝇翻译抑制因子 Pumilio(Pum),它是一类可能通过组装成有序聚集体来调节其活性的后生动物蛋白。搜索算法基于酵母朊病毒蛋白的进化序列保守模式,这些蛋白包含易聚集的谷氨酰胺/天冬酰胺(Q/N)丰富结构域,连接正常氨基酸组成的功能结构域。我们通过在酵母中表达 Pum 和其线虫同源物 PUF-9 来检测其聚集。含有 Q/N 丰富序列的 Pum 结构域(记为 NQ1)、整个 Pum N 端和完整的 PUF-9 蛋白都定位于酵母中的宏观聚集体(焦点)。NQ1 和 PUF-9 可以产生酵母 Pin+ 特性,这种特性可通过遗传聚集体传递。NQ1 也可以在体外组装成淀粉样纤维。在果蝇中,Pum 调节神经肌肉接头(NMJ)的突触后翻译。为了评估 NQ1 是否会影响体内突触 Pum 活性,我们在肌肉中表达了它。结果发现,它会负调控内源性 Pum,导致基因剂量依赖性 pum 功能丧失的 NMJ 表型。NQ1 的共表达也会抑制 Pum 在肌肉中过表达引起的致死性和 NMJ 表型。NQ1 的 Q/N 阻断是这些表型效应所必需的。NQ1 对 Pum 的负调控可能是通过形成无活性聚集体来解释的,但我们未能证明 NQ1 在果蝇中会聚集。NQ1 也可以通过“显性负”效应来调节 Pum,从而阻止 Q/N 介导的 Pum 与自身或与翻译抑制所需的辅助因子相互作用。

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本文引用的文献

1
The translational repressors Nanos and Pumilio have divergent effects on presynaptic terminal growth and postsynaptic glutamate receptor subunit composition.翻译抑制因子Nanos和Pumilio对突触前终末生长和突触后谷氨酸受体亚基组成具有不同影响。
J Neurosci. 2009 Apr 29;29(17):5558-72. doi: 10.1523/JNEUROSCI.0520-09.2009.
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Co-occupancy of two Pumilio molecules on a single hunchback NRE.单个驼背NRE上两个Pumilio分子的共同占据。
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A role for Q/N-rich aggregation-prone regions in P-body localization.富含谷氨酰胺/天冬酰胺且易于聚集的区域在P小体定位中的作用。
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Pumilio binds para mRNA and requires Nanos and Brat to regulate sodium current in Drosophila motoneurons.Pumilio结合para mRNA,并需要Nanos和Brat来调节果蝇运动神经元中的钠电流。
J Neurosci. 2008 Feb 27;28(9):2099-109. doi: 10.1523/JNEUROSCI.5092-07.2008.
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Edc3p and a glutamine/asparagine-rich domain of Lsm4p function in processing body assembly in Saccharomyces cerevisiae.Edc3p和Lsm4p富含谷氨酰胺/天冬酰胺的结构域在酿酒酵母的加工体组装中发挥作用。
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Staufen- and FMRP-containing neuronal RNPs are structurally and functionally related to somatic P bodies.含有Staufen和FMRP的神经元核糖核蛋白颗粒在结构和功能上与体细胞中的加工小体相关。
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J Neurosci. 2006 Jun 14;26(24):6496-508. doi: 10.1523/JNEUROSCI.0649-06.2006.